SUMMIT, N.J. - Thursday, March 19th 2015 [ME NewsWire]
65
percent of patients treated with GED-0301 160 mg once daily for two
weeks achieved clinical remission at both day 15 and day 28, versus 10
percent of patients on placebo
72 and 67 percent of patients treated with 160 mg once daily were in clinical remission at day 28 and at day 84, respectively
Overall rates of adverse events and serious adverse events were similar across treatment groups, including placebo
(BUSINESS
WIRE) -- Celgene Corporation (NASDAQ:CELG) today announced that results
from a double-blind, placebo-controlled, multicenter phase II trial of
three doses of GED-0301 (mongersen) in patients with active Crohn's
disease were published in the March 19 issue of The New England Journal
of Medicine.
“GED-0301 offers a unique approach to treating
Crohn’s, using antisense technology to target a key intracellular
signaling protein thought to be involved in intestinal inflammation and
the pathogenesis of the disease,” said Professor Giovanni Monteleone,
University of Rome Tor Vergata. “This orally administered therapy is
designed to act locally with its novel mechanism of action. The results
from the phase II trial suggest that GED-0301 should be studied further
in phase III trials for Crohn’s disease.”
This phase II trial
enrolled 166 adult patients with moderate-to-severe Crohn’s disease,
defined as Crohn’s Disease Activity Index (CDAI) ranging from 220 to 400
at least one week prior to enrollment, with documented inflammatory
lesions in the terminal ileum and/or right colon.
The newly
published findings from this phase II study showed that a significantly
greater proportion of patients with active Crohn’s disease achieved the
primary endpoint of clinical remission at both day 15 and day 28 with
once daily GED-0301 40 mg (55 percent) or 160 mg (65 percent) than with
GED-0301 10 mg (12 percent) or placebo (10 percent; P<0.001).
Additionally, 67 (6/9 patients) percent of patients reached
glucocorticoid-free remission at day 84 with 160 mg GED-0301 once daily,
versus 11 (1/9 patients) percent with placebo (P=0.04).
For
patients treated with GED-0301 160 mg once daily, 67 percent, 72 percent
and 67 percent were in clinical remission (had a CDAI score less than
150) on day 15, day 28 and day 84, respectively, compared with 21
percent, 14 percent and 21 percent on placebo (P<0.0001 vs. placebo,
for each time point). Similar results were seen in the GED-0301 40 mg
once daily group (58 percent, 70 percent and 63 percent, respectively).
For patients treated with GED-0301 10 mg once daily, clinical remission
was achieved by 15 percent, 29 percent and 29 percent on day 15, day 28
and day 84, respectively (P=n.s. vs. placebo).
On day 28, 37
percent, 58 percent and 72 percent of patients treated with once daily
GED-0301 10 mg, 40 mg or 160 mg once daily, respectively, achieved a
clinical response (a 100-point reduction in CDAI score; a secondary
endpoint), compared with 17 percent with placebo (P=0.04, P<0.001 and
P<0.001, respectively).
The rates of patients with at least
one adverse event (AE) in the GED-0301 groups were 49 percent, 62
percent and 49 percent for 10 mg, 40 mg and 160 mg once daily,
respectively, compared with 67 percent for the placebo group. The most
commonly reported AEs in the GED-0301 treatment groups were abdominal
pain (10-12 percent), Crohn’s disease worsening (10-15 percent), urinary
tract infection (5-15 percent) and C-reactive protein increase (5-9
percent). The rates of serious adverse events in the GED-0301 dose
groups were 7 percent, 2 percent and 2 percent for 10 mg, 40 mg and 160
mg once daily, respectively, compared with 2 percent for the placebo
group.
“A significant number of Crohn’s disease patients don’t
reach remission with current therapies and are looking for additional
options,” said Scott Smith, President of Celgene Inflammation and
Immunology. “GED-0301 offers a completely different mechanism of action
that has the potential to transform the Crohn’s treatment landscape. We
are encouraged by the phase II data and are committed to bringing
innovative medicine to patients with Crohn’s disease, starting with
advancing the phase III trial for GED-0301.”
About the Study
This
phase II trial enrolled 166 adult patients with moderate-to-severe
Crohn’s disease with documented inflammatory lesions in the terminal
ileum and/or right colon. Patients with known lesions in the stomach,
proximal small intestine, transverse colon, and/or left colon,
strictures, fistulae, perianal disease, extraintestinal manifestations,
active or recent infections or a history of malignancy were excluded.
Patients
were randomly assigned to receive treatment for two weeks with one of
three daily doses of GED-0301 (10 mg, 40 mg or 160 mg tablets, once
daily) or placebo and then evaluated for responses at days 15, 28 and
84. The primary efficacy endpoint of the study was the percentage of
patients with clinical remission, defined as a CDAI score below 150 at
day 15, which was maintained at day 28. The secondary endpoints included
clinical response defined as a reduction of CDAI score of 100 points or
70 points at day 15 and day 28.
Patients could continue
receiving stable doses of oral prednisolone (≤40 mg/day), budesonide (≤9
mg/day), or mesalamine during the 2-week treatment and/or a stable dose
of immunomodulators (e.g., azathioprine, mercaptopurine, methotrexate)
if therapy was initiated ≥6 months before treatment. Antibiotics,
steroids, immunosuppressive drugs and biologics could not be initiated
prior to study entry and during the 2-week treatment. Patients received
no treatment with anti-TNF-α antibodies or other biologics within 90
days, or antibiotics within 3 weeks of the date of their initiation into
the trial.
About GED-0301
The investigational oral
antisense therapy GED-0301 is an oligonucleotide that targets the
messenger RNA (mRNA) for Smad7, thereby reducing Smad7 protein levels.
In patients with Crohn’s disease, abnormally high levels of Smad7
interfere with TGF-β1 anti-inflammatory pathways in the gut, leading to
increased inflammation. GED-0301 is designed to act locally to reduce
Smad7 levels with negligible systemic exposure.
About Crohn’s Disease
Crohn’s
disease is an immune-mediated, chronic inflammatory condition of the
gastrointestinal tract. Estimated to affect as many as three out of
every 1,000 people in Europe and North America, the disease is becoming
more common for all ethnic groups. Symptoms of Crohn’s disease —
including abdominal pain, diarrhea, fatigue, fever, weight loss and
malnutrition — most commonly begin to appear between the ages of 13 and
30, although the disease can strike at any age. The disease may affect
any part of the GI tract, from the mouth to the anus, but most commonly
affects the end of the small bowel (the ileum) and the beginning of the
colon. The exact cause of Crohn’s disease is unknown, and there is no
cure. People with Crohn’s disease have a slightly reduced life
expectancy.
About Celgene
Celgene Corporation,
headquartered in Summit, New Jersey, is an integrated global
pharmaceutical company engaged primarily in the discovery, development
and commercialization of innovative therapies for the treatment of
cancer and inflammatory diseases through gene and protein regulation.
For more information, please visit www.celgene.com. Follow Celgene on
Twitter @Celgene, and on Pinterest and LinkedIn.
Forward-Looking Statements
This
press release contains forward-looking statements, which are generally
statements that are not historical facts. Forward-looking statements can
be identified by the words “expects,” “anticipates,” “believes,”
“intends,” “estimates,” “plans,” “will,” “outlook” and similar
expressions. Forward-looking statements are based on management’s
current plans, estimates, assumptions and projections, and speak only as
of the date they are made. We undertake no obligation to update any
forward-looking statement in light of new information or future events,
except as otherwise required by law. Forward-looking statements involve
inherent risks and uncertainties, most of which are difficult to predict
and are generally beyond our control. Actual results or outcomes may
differ materially from those implied by the forward-looking statements
as a result of the impact of a number of factors, many of which are
discussed in more detail in our Annual Report on Form 10-K and other
reports filed with the Securities and Exchange Commission.
# # #
Contacts
For inquiries, please contact:
Celgene Corporation
Investors:
Patrick E. Flanigan III,
908-673-9969
Vice President, Investor Relations
or
Media:
Catherine Cantone,
732-564-3592
Director, Corporate Communications
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